A single beta-globin locus control region element (5' hypersensitive site 2) is sufficient for developmental regulation of human globin genes in transgenic mice.

B Morley, CA Abbott, J Sharpe, J Lida, P Chan-Thomas, W. Wood

    Research output: Contribution to journalArticlepeer-review

    Abstract

    The beta-globin gene complex is regulated by an upstream locus control region (LCR) which is responsible for high-level, position-independent, erythroid-cell-specific expression of the genes in the cluster. Its role in the developmental regulation of beta-like globin gene transcription remains to be established. We have examined the effect of a single LCR element, hypersensitive site 2 (HS2), on the developmental regulation of the human fetal gamma and adult beta genes in transgenic mice. In mice bearing HS2A gamma beta and HS2G gamma A gamma-117 delta beta human globin gene constructs, switching from gamma- to beta-gene expression begins at about day 13.5 of gestation and is largely completed shortly after birth. The larger construct also demonstrates a switch in G gamma- to A gamma-gene expression during the gamma-to-beta switch similar to that observed during normal human development. We conclude that HS2 alone is sufficient for developmental regulation of the human beta-globin genes.
    Original languageEnglish
    JournalMol Cell Biol
    Volume12( 5)
    Publication statusPublished - May 1992

    Keywords

    • Aging
    • Animals
    • Crosses, Genetic
    • genetics: DNA
    • Female
    • Gene Expression Regulation
    • Genes, Regulator
    • Gestational Age
    • genetics: Globins
    • genetics: Hemoglobins
    • Humans
    • Male
    • Mice
    • Mice, Transgenic
    • Multigene Family
    • genetics: RNA
    • genetics: RNA, Messenger
    • Regulatory Sequences, Nucleic Acid
    • Restriction Mapping
    • Transcription, Genetic

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